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N-糖基化。

N-Glycosylation.

机构信息

Center for Highly Advanced Integration of Nano and Life Sciences (G-CHAIN), Gifu University, Gifu, Japan.

Institute for Glyco-core Research (iGCORE), Gifu University, Gifu, Japan.

出版信息

Adv Exp Med Biol. 2021;1325:3-24. doi: 10.1007/978-3-030-70115-4_1.

DOI:10.1007/978-3-030-70115-4_1
PMID:34495528
Abstract

N-glycosylation is a highly conserved glycan modification, and more than 7000 proteins are N-glycosylated in humans. N-glycosylation has many biological functions such as protein folding, trafficking, and signal transduction. Thus, glycan modification to proteins is profoundly involved in numerous physiological and pathological processes. The N-glycan precursor is biosynthesized in the endoplasmic reticulum (ER) from dolichol phosphate by sequential enzymatic reactions to generate the dolichol-linked oligosaccharide composed of 14 sugar residues, GlcManGlcNAc. The oligosaccharide is then en bloc transferred to the consensus sequence N-X-S/T (X represents any amino acid except proline) of nascent proteins. Subsequently, the N-glycosylated nascent proteins enter the folding step, in which N-glycans contribute largely to attaining the correct protein fold by recruiting the lectin-like chaperones, calnexin, and calreticulin. Despite the N-glycan-dependent folding process, some glycoproteins do not fold correctly, and these misfolded glycoproteins are destined to degradation by proteasomes in the cytosol. Properly folded proteins are transported to the Golgi, and N-glycans undergo maturation by the sequential reactions of glycosidases and glycosyltransferases, generating complex-type N-glycans. N-Acetylglucosaminyltransferases (GnT-III, GnT-IV, and GnT-V) produce branched N-glycan structures, affording a higher complexity to N-glycans. In this chapter, we provide an overview of the biosynthetic pathway of N-glycans in the ER and Golgi.

摘要

N-糖基化是一种高度保守的聚糖修饰,人类中有超过 7000 种蛋白质发生 N-糖基化。N-糖基化具有许多生物学功能,如蛋白质折叠、运输和信号转导。因此,蛋白质的聚糖修饰深刻参与了许多生理和病理过程。N-聚糖前体在粗面内质网(ER)中由焦磷酸多萜醇通过连续的酶反应合成,生成由 14 个糖残基组成的多萜醇连接的寡糖,即 GlcManGlcNAc。然后,寡糖通过整批转移到新生蛋白质的共有序列 N-X-S/T(X 代表脯氨酸以外的任何氨基酸)上。随后,N-糖基化的新生蛋白质进入折叠步骤,其中 N-聚糖通过招募凝集素样伴侣蛋白钙联蛋白和钙网蛋白,对获得正确的蛋白质折叠有很大贡献。尽管存在 N-糖依赖性折叠过程,但一些糖蛋白不能正确折叠,这些错误折叠的糖蛋白注定会被细胞质中的蛋白酶体降解。正确折叠的蛋白质被运送到高尔基体,N-聚糖通过糖苷酶和糖基转移酶的顺序反应进行成熟,生成复杂型 N-聚糖。N-乙酰氨基葡萄糖基转移酶(GnT-III、GnT-IV 和 GnT-V)产生分支的 N-聚糖结构,使 N-聚糖具有更高的复杂性。在本章中,我们提供了 ER 和高尔基体中 N-聚糖生物合成途径的概述。

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